接受非甾体药物治疗以延长发情周期黄体期的母猪繁殖表现。

IF 1.9 2区 农林科学 Q2 AGRICULTURE, DAIRY & ANIMAL SCIENCE
Camila R.C. Brito , Ágatha D. Cordeiro , Pricila Baldessar , Carolini Schultz , Monike Quirino , Rafael R. Ulguim , Paulo B.D. Gonçalves , Thomaz Lucia Jr. , Ivan Bianchi , Bernardo G. Gasperin
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引用次数: 0

摘要

替代母猪的同步周期性对于优化繁殖群管理至关重要,然而,口服孕激素的方案成本高昂,需要每天服用。本研究在母猪黄体期测试了两种不含孕激素的同步方案。在实验I中,在第三次发情(D0)的当天,将母猪分为三组(每组n=6):对照组,不进行处理;PGF25:其中,母猪在D12和D15接受两剂hCG(各1500 IU),在D25接受两剂量前列腺素F2α(PGF)类似物(氯前列醇钠;250µg),间隔6小时;和PGF30:其中,母猪在D12和D15接受两剂hCG(各1500 IU),在D30接受两剂PGF类似物(氯前列醇钠;250µg),间隔6小时。PGF处理与发情期表达之间的间隔PGF30比PGF25短(P 0.05),但PGF30组对母猪有效(P=0.01)。在实验II中,将母猪分为三组(每组n=12):对照组(不处理);eCG+hCG(D10上的400 IU eCG加上D12上的500 IU hCG);和hCG2(两个hCG剂量,D12和D15各1500 IU)。在D30,来自eCG+hCG和hCG2的未表达发情期的母猪接受两剂PGF类似物(各250µg,间隔6小时)。当检测到发情期时,所有的母猪都进行了受精。在D10时,所有组的血清P4浓度相似(P>0.05),在D20和D25时,在eCG+hCG和hCG2中,母猪的血清P4水平更高(P 0.05)。总之,实验I表明,PGF处理在第二次hCG处理后10天没有诱导黄体解解,但在第二次hCG应用后15天有效。此外,实验II表明eCG+hCG和hCG2都能有效延长黄体期;然而,活产仔猪的数量和总产仔数受到hCG2方案的负面影响。从这个意义上说,用eCG+hCG或hCG2治疗可能代表了一种无类固醇的方法来延长母猪的黄体期,尽管治疗的剂量和数量必须进一步研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Reproductive performance in gilts submitted to non-steroidal therapies to prolong the luteal phase of the estrous cycle

Synchronized cyclicity of replacement gilts is crucial to optimize breeding herd management, however, protocols with oral progestogen are expensive and require daily administration. This study tested two synchronization protocols without progestogens during the luteal phase in gilts. In Experiment I, on the day of the expression of the third estrus (D0), gilts were assigned to three groups (n = 6, each): control, with no treatment; PGF25: in which gilts received two doses of hCG (1,500 IU each) on D12 and D15 and two doses of a prostaglandin F2α (PGF) analogue (sodium cloprostenol; 250 µg) 6-h apart, on D25; and PGF30: in which gilts received two doses of hCG (1,500 IU each) on D12 and D15 and two doses of the PGF analogue (sodium cloprostenol; 250 µg) 6-h apart, on D30. The interval between PGF treatment and estrus expression was shorter in PGF30 than in PGF25 (P < 0.01). The PGF treatment failed to decrease serum progesterone (P4) for gilts from the PGF25 group (P > 0.05), but it was effective for gilts in the PGF30 group (P = 0.01). In Experiment II, gilts were assigned to three groups (n = 12, each): control (no treatment); eCG+hCG (400 IU eCG on D10 plus 500 IU hCG on D12); and hCG2 (two hCG doses, 1,500 IU each on D12 and D15). On D30, gilts from eCG+hCG and hCG2 that did not express estrus received two doses of the PGF analogue (250 µg each, 6-h apart). All gilts were inseminated when estrus was detected. Serum P4 concentrations were similar for all groups on D10 (P > 0.05) and greater on D20 and D25 for gilts in eCG+hCG and hCG2 (P < 0.01) than for those in the control, whereas P4 concentration was greater in hCG2 than in eCG+hCG, on both moments. The inter-estrus interval (IEI) was shorter for control gilts and intermediate for gilts in eCG+hCG, while the longest IEI was observed for gilts in hCG2 (P < 0.01). Total litter size was larger for gilts in the control (P = 0.02) compared to those in hCG2 and did not differ from the other groups for gilts in eCG+hCG (P > 0.05). In conclusion, Experiment I showed that PGF treatment did not induce luteolysis 10 days after the second hCG treatment but it was effective 15 days after the second hCG application. Additionally, Experiment II showed that both eCG+hCG and hCG2 were efficient in prolonging the luteal phase; however, number of piglets born alive and total litter size were negatively affected by the hCG2 protocol. In this sense, treatment with eCG+hCG or hCG2 may represent a steroid-free approach to prolong the luteal phase in gilts, although the doses and number of treatments must be further investigated.

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来源期刊
Domestic animal endocrinology
Domestic animal endocrinology 农林科学-奶制品与动物科学
CiteScore
5.50
自引率
4.80%
发文量
58
审稿时长
31 days
期刊介绍: Domestic Animal Endocrinology publishes scientific papers dealing with the study of the endocrine physiology of domestic animal species. Those manuscripts utilizing other species as models for clinical or production problems associated with domestic animals are also welcome. Topics covered include: Classical and reproductive endocrinology- Clinical and applied endocrinology- Regulation of hormone secretion- Hormone action- Molecular biology- Cytokines- Growth factors
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